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IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS

Delayed hypersensitivity in guinea pigs was produced by immunization. with a conjugate prepared by coupling diazotized arsanilic acid to polytyrosine. The resulting sensitivity could be demonstrated by skin test with conjugates prepared from a wide variety of tyrosine-containing proteins. Definite b...

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Detalles Bibliográficos
Autor principal: Leskowitz, Sidney
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1963
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2137600/
https://www.ncbi.nlm.nih.gov/pubmed/13929877
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author Leskowitz, Sidney
author_facet Leskowitz, Sidney
author_sort Leskowitz, Sidney
collection PubMed
description Delayed hypersensitivity in guinea pigs was produced by immunization. with a conjugate prepared by coupling diazotized arsanilic acid to polytyrosine. The resulting sensitivity could be demonstrated by skin test with conjugates prepared from a wide variety of tyrosine-containing proteins. Definite but smaller degrees of sensitivity could be induced with conjugates of proteins containing little or no tyrosine. The apparent absence of carrier-specificity is considered to be due to the narrowed range of immunologic response produced by immunization with polytyrosine-azobenzenearsonate. Injections of the hapten N-acetyltyrosine-azobenzenearsonate was found to suppress completely the delayed reaction attributable to the tyrosine-azobenzenearsonate group. The same hapten was only slightly effective in suppressing reactions in guinea pigs immunized with guinea pig serum albumin-azobenzenearsonate, suggesting that a broader range of specificities is involved with such antigens. Confirmation of such increased range of specificity attributable to antigenic determinants contributed by the carrier protein was obtained by desensitization studies with N-acetyltyrosine-azobenzenearsonate and guinea pig serum albumin-azobenzoate. While separately these materials produced only a slight decrease in skin reactivity to guinea pig serum albumin-azobenzenearsonate, the combination was found to give almost complete suppression.
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spelling pubmed-21376002008-04-17 IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS Leskowitz, Sidney J Exp Med Article Delayed hypersensitivity in guinea pigs was produced by immunization. with a conjugate prepared by coupling diazotized arsanilic acid to polytyrosine. The resulting sensitivity could be demonstrated by skin test with conjugates prepared from a wide variety of tyrosine-containing proteins. Definite but smaller degrees of sensitivity could be induced with conjugates of proteins containing little or no tyrosine. The apparent absence of carrier-specificity is considered to be due to the narrowed range of immunologic response produced by immunization with polytyrosine-azobenzenearsonate. Injections of the hapten N-acetyltyrosine-azobenzenearsonate was found to suppress completely the delayed reaction attributable to the tyrosine-azobenzenearsonate group. The same hapten was only slightly effective in suppressing reactions in guinea pigs immunized with guinea pig serum albumin-azobenzenearsonate, suggesting that a broader range of specificities is involved with such antigens. Confirmation of such increased range of specificity attributable to antigenic determinants contributed by the carrier protein was obtained by desensitization studies with N-acetyltyrosine-azobenzenearsonate and guinea pig serum albumin-azobenzoate. While separately these materials produced only a slight decrease in skin reactivity to guinea pig serum albumin-azobenzenearsonate, the combination was found to give almost complete suppression. The Rockefeller University Press 1963-06-01 /pmc/articles/PMC2137600/ /pubmed/13929877 Text en Copyright ©, 1963, by The Rockefeller Institute This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Leskowitz, Sidney
IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS
title IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS
title_full IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS
title_fullStr IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS
title_full_unstemmed IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS
title_short IMMUNOCHEMICAL STUDY OF ANTIGENIC SPECIFICITY IN DELAYED HYPERSENSITIVITY : II. DELAYED HYPERSENSITIVITY TO POLYTYROSINE-AZOBENZENEARSONATE AND ITS SUPPRESSION BY HAPTENS
title_sort immunochemical study of antigenic specificity in delayed hypersensitivity : ii. delayed hypersensitivity to polytyrosine-azobenzenearsonate and its suppression by haptens
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2137600/
https://www.ncbi.nlm.nih.gov/pubmed/13929877
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